Abiraterone plus prednisone improves survival in metastatic castration-resistant prostate cancer.

I n essentially just 1 year’s time, we have seen science translated into exciting new therapeutic agents for men with metastatic castration-resistant prostate cancer (CRPC), most recently with the United States Food and Drug Administration (FDA) approval of abiraterone acetate in combination with prednisone. While prostate cancer has been known to be highly responsive to surgical or medical castration for well over half a century, what was once termed ‘hormone refractory’ prostate cancer inevitably developed, leading to cancerrelated death. Many consider the introduction of chemotherapy for CRPC initially for symptomatic benefit, then with improvements in survival, a substantial step forward. Nonetheless, most patients experience disease progression within months. Multiple factors, including unfavorable perceptions of benefit/ toxicity ratio, therapeutic nihilism, barriers to shift in care between medical disciplines, a low percentage of patients participating in clinical trials and several ‘negative’ studies, left the field at a therapeutic standstill since 2004. It is now widely recognized that despite castrate levels of serum testosterone, most prostate tumors remain dependent on androgen receptor (AR) signaling, which can occur through AR gene amplification, activating mutations, AR promiscuity, intratumoral ligand (e.g., testosterone) production, AR bypass pathways or alternative mechanisms. Drugs such as ketoconazole, which inhibit production of adrenal precursors into testosterone (T) and dihydrotestosterone, may have clinical benefit in some patients with CRPC, but no clinical study had shown a survival benefit associated with secondary hormonal manipulations. More recently, intratumoral conversion of adrenal precursors into T and dihydrotestosterone has been identified in CRPC. Abiraterone acetate is a potent inhibitor of cytochrome P450 c17 (17a-hydroxylase/ C17,20 lyase), which inhibits conversion of androgen precursors to T and dihydrotestosterone in testes, adrenal glands and prostate tumor tissue, and is more potent and selective than ketoconazole. Phase I and II trials demonstrated relative safety and efficacy, leading to randomized, placebo-controlled phase III trials. In the recently reported trial, 1195 men with progressive metastatic CRPC who previously received docetaxel-based chemotherapy were randomized in a 2 : 1 fashion to abiraterone acetate plus prednisone versus placebo plus prednisone with the primary end point of overall survival. A preplanned interim analysis demonstrated a statistically significant and clinically meaningful improvement in overall survival from a median of 10.9–14.8 months (hazard ratio: 0.65; 95% confidence interval: 0.54–0.77), and the independent data safety monitoring board recommended release of results and unblinding of the data; subjects who received placebo were offered crossover to active drug. In addition to overall survival improvement, benefit in progression-free survival (as measured by prostate-specific antigen as well as radiographic evidence) and response rates were seen. All subgroups analyzed experienced a benefit. Further analysis demonstrated symptomatic benefit in terms of pain control and skeletal-related events. In general, abiraterone acetate is well tolerated. In the phase III study including prednisone, toxicities related to mineralocorticoid excess including hypokalemia, fluid retention, and hypertension were seen as expected based upon the mechanism of action. Most toxicities were low grade, with all grade 3 and 4 toxicities occurring in less than 10% of patients. Modest doses of corticosteroids can in part overcome the mineralocorticoid excess seen with feedback stimulation of adrenocorticotropic hormone with relative decreases in serum cortisol as the result of 17a-hydroxylase inhibition. As single-armed studies have been performed without the addition of corticosteroids, some have advocated the omission of routine corticosteroids, instead adding them on progression, often with the use of the mineralocorticoid antagonist eplerenone to decrease toxicity. Though there may be rationale, particularly should abiraterone be used at an earlier stage of disease (presumably for longer periods of time), this is in the absence of randomized data, the FDA has approved abiraterone acetate in combination with prednisone, and eplerenone is not widely available in the United States. It should be noted that spironolactone should not be substituted. In addition to the above, the practicing physician needs to be aware of significant variability in abiraterone’s absorption with food (particularly fatty food) and potential drug–drug interactions. The current FDA approval is abiraterone acetate and prednisone for men with metastatic CRPC who have previously received docetaxel. As commented upon in the accompanying editorial, should this be the case with the currently available evidence? We as clinical investigators in conjunction with the FDA created artificial ‘boxes’ based less upon biology than on convenience. While the previous quickest pathway to FDA approval was in the refractory to initial hormonal therapy and chemotherapy setting, and because of logistics or industry fears of testing new therapies head to head with docetaxel, does it make sense to deprive patients of off-label use of approved therapies that have demonstrated some level of safety and efficacy? While the placebo-controlled randomized study of abiraterone acetate in the ‘minimally Departments of Medicine and Urology, Weill Cornell Medical College, Weill Cornell Cancer Center, New York, NY 10065, USA Correspondence: Dr ST Tagawa (stt2007@ med.cornell.edu) Asian Journal of Andrology (2011) 13, 785–786 2011 AJA, SIMM & SJTU. All rights reserved 1008-682X/11 $32.00